Literature DB >> 26951260

Sox10 expression in ovarian epithelial tumors is associated with poor overall survival.

Ah-Young Kwon1, Ilyeong Heo1, Hye Jin Lee1, Gwangil Kim1,2, Haeyoun Kang1,2, Jin-Hyung Heo1,2, Tae Hoen Kim1,2, Hee Jung An3,4.   

Abstract

Sox10 is a transcription factor regulating the development of several cell lineages and is involved in tumor development. However, the clinicopathological relevance of Sox10 expression in ovarian cancer has not been examined. We assessed expression of Sox10 in ovarian epithelial tumors by immunohistochemistry and assessed its prognostic value by analyzing the correlation between its expression and clinicopathological factors. We used tissue microarrays including 244 ovarian epithelial tumors. Sox10 staining was found in the cytoplasm or nucleus of tumor cells. Malignant serous, mucinous, and endometrioid tumors were significantly more likely to express Sox10 than benign and borderline tumors. Expression patterns in adenocarcinomas were different for histologic subtypes: nuclear Sox10 staining was common in clear-cell adenocarcinomas and serous adenocarcinomas, whereas all cases of mucinous and endometrioid tumors were negative for nuclear staining. Nuclear Sox10 staining was also associated with chemoresistance and shorter overall survival in ovarian adenocarcinomas, notably in high-grade serous adenocarcinoma. Sox10 is expressed in many ovarian carcinomas, suggesting that it might be involved in oncogenesis of ovarian carcinoma. Expression pattern of Sox10 differs between histological subtypes. Nuclear Sox10 expression is an independent indicator of poor prognosis in ovarian adenocarcinomas, notably in high-grade serous adenocarcinomas.

Entities:  

Keywords:  Biomarkers; Immunohistochemistry; Ovarian neoplasm; Serous adenocarcinoma; Sox10; Survival

Mesh:

Substances:

Year:  2016        PMID: 26951260     DOI: 10.1007/s00428-016-1918-9

Source DB:  PubMed          Journal:  Virchows Arch        ISSN: 0945-6317            Impact factor:   4.064


  31 in total

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